PLoS Biology (Jan 2024)

Retinoic acid signaling regulates spatiotemporal specification of human green and red cones.

  • Sarah E Hadyniak,
  • Joanna F D Hagen,
  • Kiara C Eldred,
  • Boris Brenerman,
  • Katarzyna A Hussey,
  • Rajiv C McCoy,
  • Michael E G Sauria,
  • James A Kuchenbecker,
  • Thomas Reh,
  • Ian Glass,
  • Maureen Neitz,
  • Jay Neitz,
  • James Taylor,
  • Robert J Johnston

DOI
https://doi.org/10.1371/journal.pbio.3002464
Journal volume & issue
Vol. 22, no. 1
p. e3002464

Abstract

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Trichromacy is unique to primates among placental mammals, enabled by blue (short/S), green (medium/M), and red (long/L) cones. In humans, great apes, and Old World monkeys, cones make a poorly understood choice between M and L cone subtype fates. To determine mechanisms specifying M and L cones, we developed an approach to visualize expression of the highly similar M- and L-opsin mRNAs. M-opsin was observed before L-opsin expression during early human eye development, suggesting that M cones are generated before L cones. In adult human tissue, the early-developing central retina contained a mix of M and L cones compared to the late-developing peripheral region, which contained a high proportion of L cones. Retinoic acid (RA)-synthesizing enzymes are highly expressed early in retinal development. High RA signaling early was sufficient to promote M cone fate and suppress L cone fate in retinal organoids. Across a human population sample, natural variation in the ratios of M and L cone subtypes was associated with a noncoding polymorphism in the NR2F2 gene, a mediator of RA signaling. Our data suggest that RA promotes M cone fate early in development to generate the pattern of M and L cones across the human retina.